Vertebrates, from fish to man, have a membrane potential mediated in part by chloride ions (Cl-). One of the first neuronal activity during development of the zebrafish spinal cord is cell depolarisation mediated by chloride extrusion via glycinergic receptors (GlyRs) and GABAergic receptors. This depolarisation is due to the absence of chloride-potassium cotransport channel KCC2, whose expression comes later in development, creating a hyperpolarising gradient. The role of this paradoxal depolarisation period during early stages of development is still unknown. By injecting KCC2 mRNA in newly fertilised zebrafish embryos, we expressed this co-transporter channel in neurons causing glycine to hyperpolarize in early phases of development. We also directly targeted the glycine receptor (GlyR) itself by blocking its activation with a chronic treatment of Strychnine, a specific drug, and by knocking down the expression of this receptor with an antisense morpholino injection. In those three conditions (KCC2, Strychnine and GlyR KD), perturbation of neuronal activity provoked major defects in neurogenesis, particulary in development of interneurons, without affecting other types of cells like motoneurons and sensory neurons. In addition, blocking low-voltage activated calcium channels with nifedipine provoked similar phenotypes. We conclude that the early glycine-mediated depolarisation allow calcium entry, thus activating certain aspects of interneurons neurogenesis.